Literature DB >> 23832397

A phase l study of three different dosing schedules of the oral aurora kinase inhibitor MSC1992371A in patients with solid tumors.

M Mita1, M Gordon, N Rejeb, A Gianella-Borradori, V Jego, A Mita, J Sarantopoulos, K Sankhala, D Mendelson.   

Abstract

Aurora kinase inhibitors (AKIs) are a class of antimitotic, small-molecule anticancer agents. MSC1992371A is an AKI being evaluated for the treatment of patients with solid tumors. This phase I, open-label, dose-escalation study determined the maximum tolerated dose (MTD) of MSC1992371A in different dosing schedules in patients with locally advanced or metastatic solid tumors. MSC1992371A was administered on days 1 and 8 (schedule 1) or on days 1, 2, and 3 (schedule 2) of a 21-day cycle. The study was expanded with a third schedule (study drug on days 1-3 and 8-10). Adverse events were monitored throughout the study. Antitumor efficacy, drug pharmacokinetics, and pharmacodynamics were evaluated. Ninety-two patients were enrolled. MSC1992371A was dosed over eight levels in schedules 1 and 2, and the MTD was determined as 74 mg/m(2) per cycle for both schedules and as 60 mg/m(2) in schedule 3, albeit only in three patients due to discontinuation of the study. Overall, the most common grade 3 or 4 treatment-emergent adverse events were neutropenia, febrile neutropenia, thrombocytopenia, anemia, and fatigue. The most frequent dose-limiting toxicity over all schedules was neutropenia. MSC1992371A plasma concentrations tended to increase with increasing dose levels. Although no complete or partial responses were seen, stable disease ≥3 months was observed in 11 patients. Analysis for markers of target modulation and pharmacodynamics effects was unsuccessful. MSC1992371A was generally well tolerated in patients, with mainly transient hematologic toxicities apparent at an MTD of 60-74 mg/m(2)/21-day cycle, independent of dosing frequency.

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Year:  2013        PMID: 23832397     DOI: 10.1007/s11523-013-0288-3

Source DB:  PubMed          Journal:  Target Oncol        ISSN: 1776-2596            Impact factor:   4.493


  17 in total

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Authors:  E A Nigg
Journal:  Nat Rev Mol Cell Biol       Date:  2001-01       Impact factor: 94.444

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Journal:  Invest New Drugs       Date:  2012-06-02       Impact factor: 3.850

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Journal:  J Natl Cancer Inst       Date:  2000-02-02       Impact factor: 13.506

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6.  Phase 1 study of MLN8054, a selective inhibitor of Aurora A kinase in patients with advanced solid tumors.

Authors:  E Claire Dees; Jeffrey R Infante; Roger B Cohen; Bert H O'Neil; Suzanne Jones; Margaret von Mehren; Hadi Danaee; Yih Lee; Jeffrey Ecsedy; Mark Manfredi; Katherine Galvin; Bradley Stringer; Hua Liu; Omar Eton; Howard Fingert; Howard Burris
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Authors:  Anne M Traynor; Maureen Hewitt; Glenn Liu; Keith T Flaherty; Jason Clark; Steven J Freedman; Boyd B Scott; Ann Marie Leighton; Patricia A Watson; Baiteng Zhao; Peter J O'Dwyer; George Wilding
Journal:  Cancer Chemother Pharmacol       Date:  2010-04-13       Impact factor: 3.333

10.  Aurora B kinase inhibitor AZD1152: determinants of action and ability to enhance chemotherapeutics effectiveness in pancreatic and colon cancer.

Authors:  A Azzariti; G Bocci; L Porcelli; A Fioravanti; P Sini; G M Simone; A E Quatrale; P Chiarappa; A Mangia; S Sebastian; D Del Bufalo; M Del Tacca; A Paradiso
Journal:  Br J Cancer       Date:  2011-02-08       Impact factor: 7.640

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Journal:  Invest New Drugs       Date:  2015-05-02       Impact factor: 3.850

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Review 5.  The aurora kinases in cell cycle and leukemia.

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Journal:  Oncogene       Date:  2014-03-17       Impact factor: 9.867

6.  Inhibition of Aurora kinase B is important for biologic activity of the dual inhibitors of BCR-ABL and Aurora kinases R763/AS703569 and PHA-739358 in BCR-ABL transformed cells.

Authors:  Anna L Illert; Anna K Seitz; Christoph Rummelt; Stefanie Kreutmair; Richard A Engh; Samantha Goodstal; Christian Peschel; Justus Duyster; Nikolas von Bubnoff
Journal:  PLoS One       Date:  2014-11-26       Impact factor: 3.240

Review 7.  Targeting AURKA in Cancer: molecular mechanisms and opportunities for Cancer therapy.

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  7 in total

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